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Clinical Pharmacokinetics

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01-12-2005 | Review Article

Clinical Pharmacology of Lumiracoxib

A Selective Cyclo-Oxygenase-2 Inhibitor

Authors: Dr Christiane M. Rordorf, Les Choi, Paul Marshall, James B. Mangold

Published in: Clinical Pharmacokinetics | Issue 12/2005

Abstract

Lumiracoxib (Prexige®) is a selective cyclo-oxygenase (COX)-2 inhibitor developed for the treatment of osteoarthritis, rheumatoid arthritis and acute pain. Lumiracoxib possesses a carboxylic acid group that makes it weakly acidic (acid dissociation constant [pKa] 4.7), distinguishing it from other selective COX-2 inhibitors.

Lumiracoxib has good oral bioavailability (74%). It is rapidly absorbed, reaching maximum plasma concentrations 2 hours after dosing, and is highly plasma protein bound. Lumiracoxib has a short elimination half-life from plasma (mean 4 hours) and demonstrates dose-proportional plasma pharmacokinetics with no accumulation during multiple dosing. In patients with rheumatoid arthritis, peak lumiracoxib synovial fluid concentrations occur 3–4 hours later than in plasma and exceed plasma concentrations from 5 hours after dosing to the end of the 24-hour dosing interval. These data suggest that lumiracoxib may be associated with reduced systemic exposure, while still reaching sites where COX-2 inhibition is required for pain relief.

Lumiracoxib is metabolised extensively prior to excretion, with only a small amount excreted unchanged in urine or faeces. Lumiracoxib and its metabolites are excreted via renal and faecal routes in approximately equal amounts. The major metabolic pathways identified involve oxidation of the 5-methyl group of lumiracoxib and/or hydroxylation of its dihaloaromatic ring. Major metabolites of lumiracoxib in plasma are the 5-carboxy, 4′-hydroxy and 4′-hydroxy-5-carboxy derivatives, of which only the 4′-hydroxy derivative is active and COX-2 selective. In vitro, the major oxidative pathways are catalysed primarily by cytochrome P450 (CYP) 2C9 with very minor contribution from CYP1A2 and CYP2C19. However, in patients genotyped as poor CYP2C9 metabolisers, exposure to lumiracoxib (area under the plasma concentration-time curve) is not significantly increased compared with control subjects, indicating no requirement for adjustment of lumiracoxib dose in these subjects.

Lumiracoxib is selective for COX-2 compared with COX-1 in the human whole blood assay with a ratio of 515: 1 in healthy subjects and in patients with osteoarthritis or rheumatoid arthritis. COX-2 selectivity was confirmed by a lack of inhibition of arachidonic acid and collagen-induced platelet aggregation. COX-2 selectivity of lumiracoxib is associated with a reduced incidence of gastroduodenal erosions compared with naproxen and a lack of effect on both small and large bowel permeability.

Lumiracoxib does not exhibit any clinically meaningful interactions with a range of commonly used medications including aspirin (acetylsalicylic acid), fluconazole, an ethinylestradiol- and levonorgestrel-containing oral contraceptive, omeprazole, the antacid Maalox®, methotrexate and warfarin (although, as in common practice, routine monitoring of coagulation is recommended when lumiracoxib is co-administered with warfarin). As such, dose adjustments are not required when co-administering these agents with lumiracoxib. In addition, moderate hepatic impairment and mild to moderate renal impairment do not appear to influence lumiracoxib exposure.

The use of trade names is for product identification purposes only and does not imply endorsement.

Schnitzer TJ, Burmester GR, Mysler E, et al. TARGET Study Group. Comparison of lumiracoxib with naproxen and Ibuprofen in the Therapeutic Arthritis Research and Gastrointestinal Event Trial (TARGET), reduction in ulcer complications: randomised controlled trial. Lancet 2004; 364: 665–74PubMedCrossRef

Farkouh ME, Kirshner H, Harrington RA, et al. TARGET Study Group. Comparison of lumiracoxib with naproxen and Ibuprofen in the Therapeutic Arthritis Research and Gastrointestinal Event Trial (TARGET), cardiovascular outcomes: randomised controlled trial. Lancet 2004; 364: 675–84PubMedCrossRef

Warner TD, Mitchell JA. Cyclooxygenases: new forms, new inhibitors, and lessons from the clinic. FASEB J 2004; 18: 790–804PubMedCrossRef

Brune Hinz Selective cyclooxygenase-2 inhibitors: similarities and differences. Scand J Rheumatol 2004; 33(1): 1–6CrossRef

Mangold JB, Gu H, Rodriguez LC, et al. Pharmacokinetics and metabolism of lumiracoxib in healthy male subjects. Drug Metab Dispos 2004; 32: 566–71PubMedCrossRef

Kurumbail R, Stevens A, Gierse J, et al. Structural basis for selective inhibition of cyclooxygenase-2 by anti-inflammatory agents. Nature 1996; 384: 644–8PubMedCrossRef

Clark K, Kulathila R, Koehn J, et al. Crystal structure of the cyclooxygenase-2-lumiracoxib complex [abstract 178]. In: Book of Abstracts. Philadelphia (PA): American Chemical Society (ACS), 2004 Aug 22–26

Marshall PJ, Berry JC, Wasvary J, et al. The in vitro and in vivo selectivity of COX189, a new and highly selective inhibitor of COX-2 [abstract SAT0013]. Ann Rheum Dis 2002; 61 Suppl. 1:259

Hawkey C, Hoexter G, Richard D, et al. Lumiracoxib, a novel cyclooxygenase-2 selective inhibitor, has improved gastrointestinal safety and tolerability compared with nonselective nonsteroidal anti-inflammatory drugs: a pooled analysis [abstract 87]. Arthritis Rheum 2003; 48 Suppl. 9: 79

10.

Hawkey CJ, The PUCCINI (Prevention of Ulcers with COX189 Compared with Ibuprofen In NSAID Investigation) Study Group. Reduced cumulative incidence of gastroduodenal ulcers with two doses of a new coxib, COX189 compared with standard therapeutic doses of Ibuprofen in osteoarthritis patients [abstract WED-G-553]. Gut 2002; 51 Suppl. 3: A313

11.

Kivitz AJ, Nayiager S, Schimansky T, et al. Reduced incidence of gastroduodenal ulcers associated with lumiracoxib compared with Ibuprofen in patients with rheumatoid arthritis. Aliment Pharmacol Ther 2004; 19: 1189–98PubMedCrossRef

12.

Atherton C, Jones J, McKaig B, et al. Pharmacology and gastrointestinal safety of lumiracoxib, a novel cyclooxygenase-2 selective inhibitor: an integrated study. Clin Gastroenterol Hepatol 2004; 2: 113–20PubMedCrossRef

13.

Rordorf C, Kellett N, Mair S, et al. Gastroduodenal tolerability of lumiracoxib vs placebo and naproxen: a pilot endoscopy study in healthy male subjects. Aliment Pharmacol Ther 2003; 18: 533–41PubMedCrossRef

14.

Tannenbaum H, Berenbaum F, Reginster J-Y, et al. Lumiracoxib is effective in the treatment of osteoarthritis of the knee: a 13-week, randomized, double-blind study versus placebo and celecoxib. Ann Rheum Dis 2004; 63: 1419–26PubMedCrossRef

15.

Schell E, Boucher L, Tamasi L, et al. Long-term efficacy and tolerability of lumiracoxib in osteoarthritis of the knee [abstract FRI0224]. Ann Rheum Dis 2003; 62 Suppl. I: 264

16.

Schnitzer TJ, Beier J, Geusens P, et al. Efficacy and safety of four doses of lumiracoxib versus diclofenac in patients with knee or hip primary osteoarthritis: a phase II, four-week, multicenter, randomized, double-blind, placebo-controlled trial. Arthritis Care Res 2004; 5: 549–57CrossRef

17.

Geusens P, Alten R, Rovensky J, et al. Efficacy, safety and tolerability of lumiracoxib in patients with rheumatoid arthritis: results of a randomized double-blind study. Int J Clin Pract 2004; 58: 1033–41PubMedCrossRef

18.

Kellstein D, Ott D, Jayawardene S, et al. Analgesic efficacy of a single dose of lumiracoxib compared with rofecoxib, celecoxib and placebo in the treatment of postoperative dental pain. Int J Clin Pract 2004; 58: 244–50PubMedCrossRef

19.

Kepple JS, Scott G, Rordorf C, et al. An open label, randomized, three-period, cross over study in healthy volunteers to assess the effect of food on the bioavailability of COX189 Final Market Image tablet and to compare the bioavailability of the FMI tablet to the clinical service capsule formulation in fasted subjects. Novartis Pharma AG, 2000. (Data on file)

20.

Hartmann S, Scott G, Rordorf et al. Lumiracoxib demonstrates high absolute bioavailability in healthy subjects [abstract P-199]. In: Tulunay FC, Orme M, editors. European collaboration: towards drug development and rational drug therapy. Sixth Congress of the European Association for Clinical Pharmacology and Therapeutics; 2003 Jun 24–28; Istanbul. Berlin: Springer-Verlag, 2003: 124

21.

Scott G, Rordorf C, Blood P, et al. Dose escalation study to assess the safety, tolerability, pharmacokinetics and pharmacodynamics of COX189 in healthy subjects [abstract FRI0300]. Ann Rheum Dis 2002; 61 Suppl. I: 242

22.

Furuie H, Murakami M, Matsuguma K, et al. The evaluation of the COX-2 selective inhibition of lumiracoxib, a novel nonsteroidal anti-inflammatory drug [abstract PI-6]. Clin Pharmacol Ther 2004; 75: P5CrossRef

23.

Rordorf C, Scott G, Milosavljev S, et al. Steady state pharmacokinetics, pharmacodynamics, safety and tolerability of COX189 in healthy subjects [abstract AB0284]. Ann Rheum Dis 2002; 61 Suppl. I: 420

24.

Scott G, Rordorf C, Milosavljev S, et al. Pharmacokinetics and pharmacodynamics of COX189 in patients with knee or hip primary osteoarthritis [abstract THU0233]. Ann Rheum Dis 2002; 61 Suppl. 1: 128

25.

Scott G, Branson J, Milosavljev S, et al. Lumiracoxib demonstrates dose-proportional and time-independent pharmacokinetics in patients with osteoarthritis of the knee [abstract FRI0235]. Ann Rheum Dis 2003; 62 Suppl. I: 267

26.

Scott G, Rordorf C, Milosavljev S, et al. Multiple-dose lumiracoxib shows rapid absorption and COX-2 selectivity without accumulation in patients with rheumatoid arthritis [abstract P-197]. In: Tulunay FC, Orme M, editors. European collaboration: towards drug development and rational drug therapy. Sixth Congress of the European Association for Clinical Pharmacology and Therapeutics; 2003 Jun 24–28; Istanbul. Berlin: Springer-Verlag, 2003: 124

27.

Scott G, Rordorf C, Reynolds C, et al. Pharmacokinetics of lumiracoxib in plasma and synovial fluid. Clin Pharmacokinet 2004; 43: 467–78PubMedCrossRef

28.

Patrignani P, Campestrini J, Branson J, et al. Lumiracoxib is a selective inhibitor of cyclooxygenase-2 in patients with osteoarthritis [abstract FRI0412]. Ann Rheum Dis 2004; 63 Suppl. I: 368

29.

Kalbag J, Scott G, Perry S, et al. A single dose, open-label, parallel-group study to evaluate the pharmacokinetics of COX189A in subjects with end stage renal disease requiring hemodialysis in comparison with healthy controls. Novartis Pharma AG, 2002. (Data on file)

30.

Kalbag J, Choi L, Wang Y. A single dose, open-label, parallel-group study to evaluate the pharmacokinetics of a single 200mg COX189 dose in patients with impaired renal function compared to age, sex, and weight matched control group of healthy subjects. Novartis Pharma AG, 2004. (Data on file)

31.

Kalbag J, Yeh C-M, Milosavljev S, et al. No influence of moderate hepatic impairment on the pharmacokinetics of lumiracoxib, an oral COX-2 selective inhibitor. Pharmacol Res 2004; 50: 181–6PubMedCrossRef

32.

Scott G, Vinluan Reynolds C, Milosavljev S, et al. Lack of effect of omeprazole or of an aluminium hydroxide/magnesium hydroxide antacid on the pharmacokinetics of lumiracoxib. Clin Pharmacokinet 2004; 43: 341–8PubMedCrossRef

33.

Scott G, Yih L, Yeh CM, et al. Lumiracoxib: pharmacokinetic and pharmacodynamic profile when coadministered with fluconazole in healthy subjects. J Clin Pharmacol 2004; 44: 193–9PubMedCrossRef

34.

Jermany J, Branson J, Schmouder R, et al. Lumiracoxib does not affect the ex vivo antiplatelet aggregation of low-dose aspirin in healthy subjects. J Clin Pharmacol 2005; 45: 1172–8PubMedCrossRef

35.

Hartmann S, Scott G, Rordorf C, et al. Lumiracoxib does not affect the pharmacokinetics of methotrexate in patients with stable rheumatoid arthritis [abstract P-193]. In: Tulunay FC, Orme M, editors. European collaboration: towards drug development and rational drug therapy. Sixth Congress of the European Association for Clinical Pharmacology and Therapeutics; 2003 Jun 24–28; Istanbul. Berlin: Springer-Verlag, 2003: 123

36.

Bonner J, Branson J, Milosavljev S, et al. Co-administration of lumiracoxib and warfarin does not alter the pharmacokinetic profile of R- or S-warfarin [abstract FRI0225]. Ann Rheum Dis 2003; 62 Suppl. I: 264

37.

Kalbag J, Elder C, Scott G, et al. Concomitant administration of lumiracoxib and a triphasic oral contraceptive does not affect contraceptive activity or pharmacokinetic profile. J Clin Pharmacol 2004; 44: 646–54PubMedCrossRef

38.

Weaver M. Blood distribution and plasma and/or serum protein binding report of 14C COX189 in rat, monkey and human. Novartis Corp Inc., 1999. (Data on file)

39.

Wallis WJ, Simkin PA. Antirheumatic drug levels in human synovial fluid and synovial tissue: observations on extravascular pharmacokinetics. Clin Pharmacokinet 1983; 8: 496–522PubMedCrossRef

40.

Shire Pharmaceuticals Ltd, 2002. Lodine SR capsules UK summary of product characteristics [online]. Available from URL: http://emc.medicines.org.uk [Accessed 2005 Mar 3]

41.

Benson MD, Aldo-Benson M, Brandt KD. Synovial fluid concentrations of diclofenac in patients with rheumatoid arthritis or osteoarthritis. Semin Arthritis Rheum 1985; 15 Suppl. 1: 65–7PubMedCrossRef

42.

Scott G, Rordorf C. Summary of clinical pharmacology studies. Novartis Pharma AG, 2002. (Data on file)

43.

Kirchheiner J, Brockmöller J. Clinical consequences of cytochrome P450 2C9 polymorphism. Clin Pharmacol Ther 2005; 77: 1–16PubMedCrossRef

44.

Weaver M, Milosavljec S. In vitro plasma protein binding of COX189 and three of its metabolites. Novartis Corp Inc., 2002. (Data on file)

45.

Rordorf C, Mangold J, Krebs-Brown A, et al. A randomized, double-blind, placebo-controlled, timelagged, parallel-group, ascending single oral dose study of the safety, tolerability, pharmacokinetics and pharmacodynamics of COX189 in healthy male subjects. Novartis Pharma AG, 2002. (Data on file)

46.

Patrono C, Ciabattoni G, Pugliese F, et al. Inhibition of platelet cyclooxygenase by aspirin-like drugs: methods for in vitro and ex vivo assessment. Agents Actions Suppl 1979; 4: 138–46PubMed

47.

Brideau C, Kargman S, Liu S, et al. A human whole blood assay for clinical evaluation of biochemical efficacy of cyclooxygenase inhibitors. Inflamm Res 1996; 45: 68–74PubMedCrossRef

48.

Diclofenac US package insert. East Hanover (NJ): Novartis Pharmaceuticals Ltd, 2003

49.

Sheldon E, Beaulieu A, Paster Z, et al. Lumiracoxib 100mg once daily is an effective and well-tolerated treatment for knee Osteoarthritis: a 13-week, randomized, double-blind comparison with placebo and celecoxib. Clin Ther 2005; 27: 64–77PubMedCrossRef

50.

Decktor DL, Robinson M, Gottlieb S. Comparative effects of liquid antacids on esophageal and gastric pH in patients with heartburn. Am J Ther 1995; 2: 481–6PubMedCrossRef

51.

Guarner F. Prescribing nonsteroidal anti-inflammatory drugs together with antisecretory agents is safe but may be useless. Gastroenterology 1996; 111: 1145–6PubMedCrossRef

52.

Stewart CF, Evans WE. Drug-drug interactions with antirheumatic agents: review of selected clinically important interactions. J Rheumatol Suppl 1990; 22: 16–23PubMed

53.

Guengerich FP. Metabolism of 17 alpha-ethynylestradiol in humans. Life Sci 1990; 47: 1981–8PubMedCrossRef

54.

Wilding IR, Connor AL, Carpenter P, et al. Assessment of lumiracoxib bioavailability from targeted sites in the human intestine using remotely activated capsules and gamma scintigraphy. Pharm Res 2004; 21: 443–6PubMedCrossRef

55.

Weaver ML, Flood DJ, Kimble EF, et al. Lumiracoxib demonstrates preferential distribution to inflamed tissue in the rat following a single oral dose: an effect not seen with other cyclooxygenase-2 inhibitors [abstract AB0044]. Ann Rheum Dis 2003; 62 Suppl. I: 378

56.

Dawson J, Jagher Toscano KT, et al. Lumiracoxib shows rapid distribution to inflamed sites in a rat tissue chamber model compared with rofecoxib and celecoxib [abstract AB0042]. Ann Rheum Dis 2003; 62 Suppl. I: 377

57.

Yaksh TL, Dirig DM, Conway CM, et al. The acute antihyperalgesic action of nonsteroidal, anti-inflammatory drugs and release of spinal prostaglandin E2 is mediated by the inhibition of constitutive spinal cyclooxygenase-2 (COX-2) but not COX-1. J Neurosci 2001; 21(16): 5847–53PubMed

58.

Catella-Lawson F, McAdam B, Morrison BW, et al. Effects of specific inhibition of cyclooxygenase-2 on sodium balance, hemodynamics, and vasoactive eicosanoids. J Pharmacol Exp Ther 1999; 289: 735–41PubMed

59.

McAdam BF, Catella-Lawson I, Mardini IA, et al. Systemic biosynthesis of prostacyclin by cyclooxygenase (COX-2): the human pharmacology of a selective inhibitor. Proc Natl Acad Sci U S A 1999; 96: 272–7PubMedCrossRef

60.

Dilger Herrlinger Peters J, et al. Effects of celecoxib and diclofenac on blood pressure, renal function and vasoactive prostanoids in young and elderly subjects. J Clin Pharmacol 2002; 42: 985–94

61.

Etoricoxib UK prescribing information. Hoddesdon, Hertfordshire: Merck Sharp & Dohme Ltd, 2005

62.

Rofecoxib US prescribing information. Whitehouse Station (NJ): Merck & Co., Inc., 2004

63.

Celecoxib US prescribing information. New York: Pfizer Inc., 2005

64.

Valdecoxib US prescribing information. New York: Pfizer Inc., 2004

65.

Walter M, Jacob R, Day C, et al. Sulfone COX-2 inhibitors increase susceptibility of human LDL and plasma to oxidative modification: comparison to sulphonamide COX-2 inhibitors and NSAIDs. Atherosclerosis 2004; 177: 235–43PubMedCrossRef

Title: Clinical Pharmacology of Lumiracoxib
A Selective Cyclo-Oxygenase-2 Inhibitor
Authors: Dr Christiane M. Rordorf
Les Choi
Paul Marshall
James B. Mangold
Publication date: 01-12-2005
Publisher: Springer International Publishing
Published in: Clinical Pharmacokinetics / Issue 12/2005
Print ISSN: 0312-5963
Electronic ISSN: 1179-1926
DOI: https://doi.org/10.2165/00003088-200544120-00004

Keynote webinar | Spotlight on medication adherence

Springer Medicine

Clinical Pharmacology of Lumiracoxib

A Selective Cyclo-Oxygenase-2 Inhibitor

Abstract

Keynote webinar | Spotlight on medication adherence

Springer Medicine

Abstract

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